TY - JOUR
T1 - The SMAD-binding domain of SKI
T2 - A hotspot for de novo mutations causing Shprintzen-Goldberg syndrome
AU - Schepers, Dorien
AU - Doyle, Alexander J.
AU - Oswald, Gretchen
AU - Sparks, Elizabeth
AU - Myers, Loretha
AU - Willems, Patrick J.
AU - Mansour, Sahar
AU - Simpson, Michael A.
AU - Frysira, Helena
AU - Maat-Kievit, Anneke
AU - Van Minkelen, Rick
AU - Hoogeboom, Jeanette M.
AU - Mortier, Geert R.
AU - Titheradge, Hannah
AU - Brueton, Louise
AU - Starr, Lois
AU - Stark, Zornitza
AU - Ockeloen, Charlotte
AU - Lourenco, Charles Marques
AU - Blair, Ed
AU - Hobson, Emma
AU - Hurst, Jane
AU - Maystadt, Isabelle
AU - Destrée, Anne
AU - Girisha, Katta M.
AU - Miller, Michelle
AU - Dietz, Harry C.
AU - Loeys, Bart
AU - Van Laer, Lut
N1 - Publisher Copyright:
© 2015 Macmillan Publishers Limited All rights reserved.
PY - 2015/2/20
Y1 - 2015/2/20
N2 - Shprintzen-Goldberg syndrome (SGS) is a rare, systemic connective tissue disorder characterized by craniofacial, skeletal, and cardiovascular manifestations that show a significant overlap with the features observed in the Marfan (MFS) and Loeys-Dietz syndrome (LDS). A distinguishing observation in SGS patients is the presence of intellectual disability, although not all patients in this series present this finding. Recently, SGS was shown to be due to mutations in the SKI gene, encoding the oncoprotein SKI, a repressor of TGFβ activity. Here, we report eight recurrent and three novel SKI mutations in eleven SGS patients. All were heterozygous missense mutations located in the R-SMAD binding domain, except for one novel in-frame deletion affecting the DHD domain. Adding our new findings to the existing data clearly reveals a mutational hotspot, with 73% (24 out of 33) of the hitherto described unrelated patients having mutations in a stretch of five SKI residues (from p.(Ser31) to p.(Pro35)). This implicates that the initial molecular testing could be focused on mutation analysis of the first half of exon 1 of SKI. As the majority of the known mutations are located in the R-SMAD binding domain of SKI, our study further emphasizes the importance of TGFβ signaling in the pathogenesis of SGS.
AB - Shprintzen-Goldberg syndrome (SGS) is a rare, systemic connective tissue disorder characterized by craniofacial, skeletal, and cardiovascular manifestations that show a significant overlap with the features observed in the Marfan (MFS) and Loeys-Dietz syndrome (LDS). A distinguishing observation in SGS patients is the presence of intellectual disability, although not all patients in this series present this finding. Recently, SGS was shown to be due to mutations in the SKI gene, encoding the oncoprotein SKI, a repressor of TGFβ activity. Here, we report eight recurrent and three novel SKI mutations in eleven SGS patients. All were heterozygous missense mutations located in the R-SMAD binding domain, except for one novel in-frame deletion affecting the DHD domain. Adding our new findings to the existing data clearly reveals a mutational hotspot, with 73% (24 out of 33) of the hitherto described unrelated patients having mutations in a stretch of five SKI residues (from p.(Ser31) to p.(Pro35)). This implicates that the initial molecular testing could be focused on mutation analysis of the first half of exon 1 of SKI. As the majority of the known mutations are located in the R-SMAD binding domain of SKI, our study further emphasizes the importance of TGFβ signaling in the pathogenesis of SGS.
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U2 - 10.1038/ejhg.2014.61
DO - 10.1038/ejhg.2014.61
M3 - Article
C2 - 24736733
AN - SCOPUS:84921416171
SN - 1018-4813
VL - 23
SP - 224
EP - 228
JO - European Journal of Human Genetics
JF - European Journal of Human Genetics
IS - 2
ER -